Kmieciak Maciej, Knutson Keith L, Dumur Catherine I, Manjili Masoud H
Department of Microbiology & Immunology , VCU School of Medicine, Massey Cancer Center, Richmond, VA 23298, USA.
Eur J Immunol. 2007 Mar;37(3):675-85. doi: 10.1002/eji.200636639.
Induction of tumor-specific immune responses results in the inhibition of tumor development. However, tumors recur because of the tumor immunoediting process that facilitates development of escape mechanisms in tumors. It is not known whether tumor escape is an active process whereby anti-tumor immune responses induce loss or downregulation of the target antigen in the antigen-positive clones. To address this question, we used rat neu-overexpressing mouse mammary carcinoma (MMC) and its relapsed neu antigen-negative variant (ANV). ANV emerged from MMC under pressure from neu-specific T cell responses in vivo. We then cloned residual neu antigen-negative cells from MMC and residual neu antigen-positive cells from ANV. We found marked differences between these neu-negative clones and ANV, demonstrating that the residual neu-negative clones are probably not the origin of ANV. Since initial rejection of MMC was associated with the presence of IFN-gamma-secreting T cells, we treated MMC with IFN-gamma and showed that IFN-gamma could induce downregulation of neu expression in MMC. This appears to be due to methylation of the neu promoter. Together, these data suggest that neu antigen loss is an active process that occurs in primary tumors due to the neu-targeted anti-tumor immune responses.
诱导肿瘤特异性免疫反应可导致肿瘤发展受到抑制。然而,肿瘤会复发,这是因为肿瘤免疫编辑过程促进了肿瘤逃逸机制的发展。目前尚不清楚肿瘤逃逸是否是一个主动过程,即抗肿瘤免疫反应是否会诱导抗原阳性克隆中的靶抗原丢失或下调。为了解决这个问题,我们使用了过表达大鼠neu的小鼠乳腺癌(MMC)及其复发的neu抗原阴性变体(ANV)。ANV是在体内neu特异性T细胞反应的压力下从MMC中产生的。然后,我们从MMC中克隆了残留的neu抗原阴性细胞,并从ANV中克隆了残留的neu抗原阳性细胞。我们发现这些neu阴性克隆与ANV之间存在显著差异,这表明残留的neu阴性克隆可能不是ANV的起源。由于MMC的初始排斥反应与分泌IFN-γ的T细胞的存在有关,我们用IFN-γ处理MMC,结果表明IFN-γ可诱导MMC中neu表达的下调。这似乎是由于neu启动子的甲基化所致。总之,这些数据表明neu抗原丢失是一个主动过程,它发生在原发性肿瘤中是由于针对neu的抗肿瘤免疫反应。
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